370 likes | 1.47k Views
OAT Trial. Occluded Artery Trial (OAT). Presented at The American Heart Association Scientific Session 2006 Presented by Dr. Judith S. Hochman. OAT Trial: Background.
E N D
OAT Trial Occluded Artery Trial (OAT) Presented at The American Heart Association Scientific Session 2006 Presented by Dr. Judith S. Hochman
OAT Trial: Background • The goal of the trial was to evaluate percutaneous coronary intervention (PCI) compared with medical therapy among stable, high-risk patients with persistent total occlusion of the infarct-related artery post-myocardial infarction (MI). Presented at AHA 2006
OAT Trial: Hypothesis • A strategy of routine PCI for total occlusion of the infarct-related artery 3-28 days after acute MI would reduce the occurrence of the composite of death, reinfarction, or New York Heart Association (NYHA) class IV heart failure. Presented at AHA 2006
OAT Trial: Study Design 2166 patients with angiography on day 3-28 post-MI with evidence of total occlusion of the infarct-related artery with poor or absent antegrade flow (TIMI flow grade 0 or 1); and met a criterion for increased risk, defined as ejection fraction <50%, proximal occlusion of a major epicardial vessel with a large risk region, or both Exclusions: NYHA class III or IV heart failure, shock , serum creatinine concentration >2.5 mg/dl, angiographically significant left main or three-vessel coronary artery disease, angina at rest, or severe ischemia on stress testing. Randomized. 22% female, mean age 59 years, mean follow-up 3 years, mean EF 48% at baseline Concomitant medications: Aspirin, anticoagulation if indicated, ACE inhibitors, beta-blockers, and lipid-lowering therapy, unless contraindicated Medical Therapy n=1084 PCI with stenting n=1082 • Primary Endpoints: Death, MI, or NYHA class IV heart failure Presented at AHA 2006
OAT Trial: Primary Endpoint Primary Endpoint of death, reinfarction, NYHA class IV heart failure (% patients) Hazard Ratio 1.16, p=0.20 • The primary endpoint of death, reinfarction, or NYHA class IV heart failure occurred in 17.2% of the PCI group and 15.6% of the medical therapy group ([HR] 1.16, p=0.20). Presented at AHA 2006
OAT Trial: Primary Component Endpoints Primary Component Endpoints (% patients) • Total reinfarction trended higher in the PCI group (7.0% vs. 5.3%, HR 1.36, p=0.13), as did nonfatal reinfarction (6.9% vs. 5.0%, HR 1.44, p=0.08). • Repeated elevation of cardiac biomarkers within 48 hours of randomization occurred significantly more frequently in the PCI group (10.0% vs. 3.3%, p<0.001). • There was no difference in the individual endpoints of death (9.1% for PCI vs. 9.4% for medical therapy, p=0.83) or NYHA class IV heart failure (4.4% vs. 4.5%, p=0.92) between the treatment groups. p<0.001 p=0.83 p=0.13 p=0.08 p=0.92 % patients Total Reinfarction Nonfatal Reinfarction Repeated ↑ of Cardiac Biomarkers Death NYHA Class IV Heart Failure Presented at AHA 2006
OAT Trial: Summary • Among stable, high-risk patients with persistent total occlusion of the infarct-related artery post-MI, performance of PCI 3-28 days post-MI was not associated with a difference in the composite of death, reinfarction, or NYHA class IV heart failure through a mean follow-up of 3 years compared with medical therapy. • Despite no reduction in the composite endpoint, PCI was associated with a trend toward higher rates of reinfarction compared with medication therapy. Presented at AHA 2006
OAT Trial: Summary (cont.) • The reinfarctions were not only procedural-related infarcts (i.e., early procedural enzymatic leaks), but true ST elevation reinfarctions that accumulated throughout follow-up. • One explanation for the trend toward an increase in reinfarctions with PCI may be embolization resulting in myocardial damage and impaired collateral flow. • Presence of persistent total occlusion remains a problem for a sizeable cohort of patients for whom suitable treatment is lacking. Presented at AHA 2006
OAT Trial: Summary (cont.) • Early reperfusion therapy, the goal of ST elevation MI treatment, with either primary PCI or thrombolysis, is not indicated for patients who present late, often with persistent total occlusion. • The present study, the largest randomized trial to date in this population, does not support the use of late PCI for stable but persistent total occlusion. Presented at AHA 2006